Juvenile-onset Sporadic Amyotrophic Lateral Sclerosis with a Frameshift &lt;i&gt;FUS&lt;/i&gt; Gene Mutation Presenting Unique Neuroradiological Findings and Cognitive Impairment

Hirayanagi, Kimitoshi; Sato, Masayuki; Furuta, Natsumi; Makioka, Kouki; Ikeda, Yoshio

doi:10.2169/internalmedicine.55.5569

Cited by 12 publications

(12 citation statements)

References 31 publications

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“…It is well accepted that severe clinical phenotype and aggressive course are associated with JALS patients carrying FUS mutations. In reviewing previous literatures, we found that the disease progression of JALS patients with FUS mutation in the present study is dramatically slower (a mean disease duration of 58.2 months) than previously reported JALS cases harboring FUS mutations with an average disease duration of 16.32 ± 8.65 months (Table ). Other factors may affect the estimation of survival time, such as the delayed time between onset of symptoms and diagnosis of ALS, and the intervention time of mechanical ventilation.…”

Section: Discussionsupporting

confidence: 61%

“…Other as yet unidentified factors that may influence the interfamilial phenotypic variation need to be further explored in JALS.It is well accepted that severe clinical phenotype and aggressive course are associated with JALS patients carrying FUS mutations. In reviewing previous literatures, we found that the disease progression of JALS patients with FUS mutation in the present study is dramatically slower (a mean disease duration of 58.2 months) than previously reported JALS cases harboring FUS mutations with an average disease duration of 16.32 AE 8.65 months3,[11][12][13][14][21][22][23][24][25][26][27][28][29][30][31]…”

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confidence: 99%

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The investigation of genetic and clinical features in Chinese patients with juvenile amyotrophic lateral sclerosis

et al. 2017

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Juvenile amyotrophic lateral sclerosis (JALS) occurs at an age of onset below 25 years with a heterogeneous disease onset location, variable progression and survival time. To investigate whether an ALS gene profile could resolve any aspects of clinical symptom heterogeneity, we have used targeted sequencing technology in a cohort of 12 JALS patients of Chinese descent. We detected 5 likely pathogenic mutations, 2 in familial probands and 3 in sporadic patients. One was a known TARDBP mutation (p.G348V) and 4 were FUS frameshift mutations including a known p.Gln519Ilefs*9 mutation and 3 novel mutations, p.Gly515Valfs*14, p.Gly486Profs*30, and p.Arg498Alafs*32. Of the 4 FUS mutations, 2 were able to be confirmed as de novo mutations. The TARDBP mutation carrier showed a classic ALS phenotype. All patients with FUS mutations experienced limb weakness at an early age and developed bulbar symptoms during the disease course. FUS mutations have previously been associated with increased JALS disease progression, however, we found a large range 12 to 84 months in disease survival (mean 58.2 months). Our results justify future screening for variants in FUS as it remains the most frequent genetic determinant of early onset, JALS (found in 30% of our patients).

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Section: Discussionsupporting

confidence: 61%

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confidence: 99%

The investigation of genetic and clinical features in Chinese patients with juvenile amyotrophic lateral sclerosis

et al. 2017

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“…FUS proteinopathy defines the majority of tau- and TDP-43-negative cases of frontotemporal dementia ( Urwin et al, 2010 ). Several FUS mutations have been reported to be linked to familial ALS with features of frontotemporal dementia ( Yan et al, 2010 ), and juvenile-onset ALS with cognitive impairment ( Hirayanagi et al, 2016 ). To explore the molecular mechanism underlying FUS proteinopathy in FTD, we examined tg mice overexpressing Myc-tagged exogenous ΔNLS-FUS under Thy-1 promoter, which developed progressive motor weakness from 20 weeks of age and formed ubiquitin/p62-positive cytoplasmic aggregates from 6 months of age ( Shiihashi et al, 2016 ).…”

Section: Resultsmentioning

confidence: 99%

Dendritic Homeostasis Disruption in a Novel Frontotemporal Dementia Mouse Model Expressing Cytoplasmic Fused in Sarcoma

et al. 2017

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Cytoplasmic aggregation of fused in sarcoma (FUS) is detected in brain regions affected by amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD), which compose the disease spectrum, FUS proteinopathy. To understand the pathomechanism of ALS-FTD-associated FUS, we examined the behavior and cellular properties of an ALS mouse model overexpressing FUS with nuclear localization signal deletion. Mutant FUS transgenic mice showed hyperactivity, social interactional deficits, and impaired fear memory retrieval, all of which are compatible with FTD phenotypes. Histological analyses showed decreased dendritic spine and synaptic density in the frontal cortex before neuronal loss. Examination of cultured cells confirmed that mutant but not wild-type FUS was associated with decreased dendritic growth, mRNA levels, and protein synthesis in dendrites. These data suggest that cytoplasmic FUS aggregates impair dendritic mRNA trafficking and translation, in turn leading to dendritic homeostasis disruption and the development of FTD phenotypes.

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“…FUS and UBQLN2 mutations have been linked with adult-onset ALS with frontotemporal dementia, 27 , 28 but only the first type is allegedly associated with mental retardation in JALS reports. 29 , 30 A JALS/dementia cluster has also been described in Dutch patients, corresponding to an unidentified autosomal recessive form (OMIM %205200). 31 , 32 Regarding behavioral changes, JALS type 2 patients had features of pseudobulbar affect in a Tunisian family.…”

Section: Cognitive Dysfunction In Other Motor-neuron Disordersmentioning

confidence: 97%

Cognitive dysfunction in hereditary spastic paraplegias and other motor neuron disorders

Faber

Branco

Júnior

2016

Dement. neuropsychol.

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Hereditary spastic paraplegia (HSP) is a diverse group of single-gene disorders that share the predominant clinical feature of progressive lower limb spasticity and weakness. More than 70 different genetic subtypes have been described and all modes of inheritance are possible. Intellectual dysfunction in HSP is frequent in recessive forms but rare in dominant families. It may manifest by either mental retardation and/or cognitive decline. The latter may be subtle, restricted to executive dysfunction or may evolve to severe dementia. The cognitive profile is thought to depend largely on the genetic subtype of HSP, although wide phenotypic variability within the same genetic subtype and also within the same family can be found.

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Juvenile-onset Sporadic Amyotrophic Lateral Sclerosis with a Frameshift <i>FUS</i> Gene Mutation Presenting Unique Neuroradiological Findings and Cognitive Impairment

Cited by 12 publications

References 31 publications

The investigation of genetic and clinical features in Chinese patients with juvenile amyotrophic lateral sclerosis

The investigation of genetic and clinical features in Chinese patients with juvenile amyotrophic lateral sclerosis

Dendritic Homeostasis Disruption in a Novel Frontotemporal Dementia Mouse Model Expressing Cytoplasmic Fused in Sarcoma

Cognitive dysfunction in hereditary spastic paraplegias and other motor neuron disorders

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